Analysis of whole genome sequenced cases and controls shows that the association of variants in TOMM40, BCAM, NECTIN2 and APOC1 with late onset Alzheimer's disease is driven by linkage disequilibrium with APOE ε2/ε3/ε4 alleles.

IF 1.8 4区 医学 Q3 GENETICS & HEREDITY Journal of neurogenetics Pub Date : 2021-03-01 Epub Date: 2021-05-10 DOI:10.1080/01677063.2020.1866569
David Curtis
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Abstract

Variants in APOE are associated with risk of late onset Alzheimer's disease (LOAD) but the magnitude of the effect has been reported to vary across ancestries. Also, other variants in the region have been reported to show association though it has been unclear whether this was secondary to their linkage disequilibrium with the APOE variants rs429358 and rs7412. Previous analyses of exome-sequenced samples have identified other genes in which rare variants impact risk of disease. In this study 2000 whole genome sequenced cases and controls with different ancestries were subjected to gene-based weighted burden analysis to identify risk genes. Additionally, individual variants in the APOE region were tested for association with LOAD. When using the APOE variants as covariates no individual genes showed statistically significant evidence for association after Bonferroni correction for multiple testing, which may well be a consequence of the modest sample size. Likewise, for those variants initially showing evidence of association with LOAD incorporating the APOE variants as covariates dramatically reduced the strength of association. These results demonstrate that the differential association of APOE across ancestries does not appear to be driven by another variant in the region. It seems likely that no other genes in the region have a direct effect on LOAD risk.

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对全基因组测序病例和对照组的分析表明,TOMM40、BCAM、NECTIN2 和 APOC1 中的变异与晚发性阿尔茨海默病的关联是由与 APOE ε2/ε3/ε4 等位基因的连锁不平衡驱动的。
APOE 变异与晚发性阿尔茨海默病(LOAD)的风险有关,但据报道,不同血统的影响程度不同。此外,据报道该区域的其他变异也显示出相关性,但尚不清楚这是否与 APOE 变异 rs429358 和 rs7412 的连锁不平衡有关。以前的外显子组测序样本分析发现了罕见变异影响疾病风险的其他基因。在这项研究中,对 2000 个不同血统的全基因组测序病例和对照组进行了基于基因的加权负担分析,以确定风险基因。此外,还检测了 APOE 区域的单个变异与 LOAD 的关联。当使用 APOE 变体作为协变量时,经 Bonferroni 多重检验校正后,没有单个基因显示出统计学上显著的关联证据,这很可能是样本量不大的结果。同样,对于那些最初显示出与 LOAD 相关的变体,将 APOE 变体作为协变量大大降低了相关性的强度。这些结果表明,不同祖先间 APOE 的不同关联性似乎并不是由该区域的另一个变体驱动的。看来,该地区的其他基因很可能对 LOAD 风险没有直接影响。
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来源期刊
Journal of neurogenetics
Journal of neurogenetics 医学-神经科学
CiteScore
4.40
自引率
0.00%
发文量
13
审稿时长
>12 weeks
期刊介绍: The Journal is appropriate for papers on behavioral, biochemical, or cellular aspects of neural function, plasticity, aging or disease. In addition to analyses in the traditional genetic-model organisms, C. elegans, Drosophila, mouse and the zebrafish, the Journal encourages submission of neurogenetic investigations performed in organisms not easily amenable to experimental genetics. Such investigations might, for instance, describe behavioral differences deriving from genetic variation within a species, or report human disease studies that provide exceptional insights into biological mechanisms
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